Lipases at interfaces: A review

脂肪酶 化学 脂解 基质(水族馆) 生物催化 变性(裂变材料) 水解 催化作用 酶催化 甘油三酯酶 有机化学 生物化学 反应机理 生物 脂肪组织 核化学 生态学
作者
Pablo Victor Mendes dos Reis,Krister Holmberg,Heribert J. Watzke,Martin E. Leser,R. Miller
出处
期刊:Advances in Colloid and Interface Science [Elsevier BV]
卷期号:147-148: 237-250 被引量:776
标识
DOI:10.1016/j.cis.2008.06.001
摘要

Lipases are acyl hydrolases that play a key role in fat digestion by cleaving long-chain triglycerides into polar lipids. Due to an opposite polarity between the enzyme (hydrophilic) and their substrates (lipophilic), lipase reaction occurs at the interface between the aqueous and the oil phases. Hence, interfaces are the key spots for lipase biocatalysis and an appropriate site for modulating lipolysis. Surprisingly enough, knowledge about the effects of the interfacial composition on lipase catalysis is still limited and only described by the term "interfacial quality". Recent systematic studies based on a biophysical approach allowed for the first time to show the effects of the interfacial microenvironment on lipase catalysis. These studies demonstrate that lipase activity as a function of interfacial composition is more attributed to substrate inaccessibility rather than to enzyme denaturation or inactivation, as it is often hypothesized. A detailed analysis of the interfacial properties of all compounds involved in triglyceride digestion revealed that lipolysis is a self-regulated reaction. This feedback mechanism can be explored as a new avenue to control lipase catalysis. To substantiate this hypothesis, oil hydrolysis in a model gastro-intestinal system was performed, which can be seen as an interfacial engineering approach to enzyme reactivity control. The presented characterization of the interfacial composition and its consequences provide a new approach for the understanding of lipase reactions at interfaces with direct impact on biotechnological and health care applications.
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